Tissue plasminogen activator variant uses

Title: Tissue plasminogen activator variant uses.Abstract: A method is disclosed for using tenecteplase to restore function in dysfunctional hemodialysis catheters, which have a blood flow rate of less than 300 mL/minute. Kits are also provided with instructions to direct the user to administer tenecteplase in a total dose of about 3 to 4 mg locally into all catheter lumens and allow the tenecteplase to dwell in the catheter for from about one hour to about 72 hours. ...

BACKGROUND OF THE INVENTION

This invention relates to the use of a tissue-plasminogen activator variant for restoring function in dysfunctional hemodialysis catheters.

2. Description of Related Disclosures

Plasminogen activators are enzymes that cleave the peptide bond of plasminogen between amino acid residues 561 and 562, converting it to plasmin. Plasmin is an active serine proteinase that degrades various proteins, including fibrin.

Tenecteplase (TNK, TNKASE™, Genentech, Inc., South San Francisco, Calif.), a tissue-plasminogen activator, is a sterile, purified glycoprotein of 527 amino acids resulting from modifications of the complementary DNA for natural human tissue plasminogen activator. The modifications yielded a molecule with amino acid substitutions at three sites: the substitution of asparagine for threonine 103, the substitution of glutamine for asparagine 117, and a tetra-alanine substitution at amino acids 296-299 (lysine, histidine, arginine, and arginine). Tenecteplase is a serine protease that converts plasminogen to plasmin in the presence of fibrin, with limited conversion of plasminogen to plasmin in the absence of fibrin. Tenecteplase binds to fibrin in a thrombus and converts plasminogen to plasmin. This initiates local proteolysis of fibrin associated with the thrombus with limited proteolysis of systemic fibrinogen. Tenecteplase has the same mechanism of action as alteplase and has been shown to be potent and effective in promoting clot lysis in vitro (Refino et al., Thromb Haemost, 69(6):841 (1993); Keyt et al. Proc Natl Acad Sci. USA 91:3670-4 (1994).

In human clinical trials for treatment of acute myocardial infarction (AMI), tenecteplase demonstrated similar efficacy to alteplase, but major blood loss was reduced by 22%, need for blood transfusion was reduced by 23%, and minor bleeding decreased by 16% (Assessment of the Safety and Efficacy of a New Thrombolytic Investigators (ASSENT-2). Single-bolus tenecteplase compared with front-loaded alteplase in acute myocardial infarction: the ASSENT-2 double blind randomized trial. Lancet, 354: 716-722 (1999)). There was no significant difference in the rate of intracranial hemorrhage (0.9%). Subjects with an AMI within 6 hours of symptom onset were eligible for this study. The primary objective was to compare the mortality of subjects 30 days after treatment. Safety endpoints included rates of stroke, in-hospital myocardial reinfarction or pulmonary edema/cardiogenic shock, intracranial hemorrhage (ICH), major bleeding (defined as bleeding requiring blood transfusion or leading to hemodynamic compromise), and serious bleeding events. In the group of 16,949 subjects with AMI who were evaluated, there was no difference in the mortality rate at 30 days between tenecteplase and alteplase. In addition, there was no difference in ICH rate between tenecteplase- and alteplase-treated subjects (0.93% vs. 0.94%, respectively). However, there were significantly fewer non-cerebral major bleeding events in tenecteplase- versus alteplase-treated subjects (4.66% vs. 5.94%, respectively; p-value=0.0002), and fewer transfusions (4.25% vs. 5.49%, respectively; p=0.0002). Allergic-type reactions (e.g., anaphylaxis, angioedema, laryngeal edema, rash, and urticaria) were reported in <1% of subjects treated with tenecteplase. Anaphylaxis was reported in <0.1% of subjects treated with tenecteplase; however, causality was not established.

As a result of this study, tenecteplase is currently approved for use in the reduction of mortality associated with acute myocardial infarction (AMI) in weight-tiered doses ranging from 30 to 50 mg and given as a single intravenous bolus. Because of the superior safety profile seen in AMI and its increased clot lysis efficiency, investigators have been exploring the use of tenecteplase in non-coronary applications as an alternative thrombolytic agent (Semba et al., Tech. Vasc. Interv. Radiol., (2001), supra; Sze et al., J. Vasc. Interv. Radiol., 12: 1456-1457 (2001); Razavi et al., J. Vasc. Interv. Radiol., 13: (2), Part 2: S11 (February 2002); Nehme et al., J. Vasc. Interv. Radiol., 13: S109 (2002)).

Allie et al., Tenecteplase in Peripheral Thrombolysis: Initial Safety and Feasibility Experience, abstract 48 of Society of Interventional Radiology, March 2003 (page S17) discloses that continuous tenecteplase infusion (0.25 to 0.50 mg/hour) is a safe and feasible treatment for peripheral chemical thrombolysis. Further, tenecteplase diluted to a 0.0125 mg/ml solution was found to be a feasible treatment for thrombolysing occluded peripheral arteries and veins, with only moderate effect on fibrinogen levels (Burkart et al., J. Vasc. Interv. Radiol., 13: 1099-1102 (2002)), and when combined with eptifibatide, was found to be a feasible treatment for thrombolysing acute peripheral arterial and venous occlusions (Burkart et al., J. Vasc. Interv. Radiol., 14: 729-733 (2003)). Nehme et al., J. Vasc Intery Radiol, 13:S109 (2002) presented preliminary results of a study that evaluated the efficacy of tenecteplase in de-clotting 21 thrombosed arteriovenous polytetrafluoroethylene HD grafts in 14 subjects. Using a lyse-and-wait technique, tenecteplase at 2 mg and heparin at 3000 U were injected into the grafts via an angiocatheter. The duration of drug treatment was not published, but the authors stated that the mean procedural time was 65 minutes. Technical success, defined as complete graft recanalization, was 95% (20 of 21 grafts), and clinical success, defined as one successful HD after treatment, was 90% (19 of 21). Prior to additional mechanical thrombolysis, pulse was restored in 28% of the grafts (6 of 21). The authors reported one minor bleeding event at a previous graft puncture site.

Abbas et al. J. Amer. Coll. Cardiol., 46: 793-8 (2005) evaluated the safety and efficacy of intracoronary thrombolysis in 85 subjects with chronic total occlusion for >3 months and in whom a prior attempt at recanalization with percutaneous coronary intervention (PCI) was unsuccessful. Subjects received either a weight-adjusted dose (2-5 mg/hr) of alteplase (n=61) or a standard dose (0.5 mg/hr) of tenecteplase (n=24) for 8 hours, followed by PCI; the total dose was divided between the guide catheter and a 3-French intracoronary infusion catheter. Following intracoronary thrombolysis, recanalization was achieved in 54% of all subjects (both treatment groups combined) on repeat PCI. By multivariate analysis, lesion tapering and lack of bridging collaterals were the only predictors of success. Adverse events included hematoma (8% of all subjects) and bleeding requiring transfusion (3.5% of all subjects).

Tenecteplase is available in a commercially supplied 50-mg vial and approved for a single-bolus administration in patients with AMI (TNKASE™. Full prescribing information, 2002 Physicians Desk Reference, Thomas Medical Economics Co., Montvale, N.J.). When used in approved indications, tenecteplase is reconstituted in sterile water to achieve a final concentration of 5 mg/mL and administered intravenously as a single weight-adjusted bolus.

CATHFLO®ACTIVASE® (alteplase) is indicated for the restoration of function to central venous access (CVA) devices as assessed by the ability to withdraw blood. Approval was based on two pivotal Genentech-sponsored clinical trials of alteplase for the restoration of catheter function in adult and pediatric subjects over the age of two. Subsequently, a third trial in pediatric subjects (<17 years of age, including some <2 years of age) was performed. All three studies, whether placebo-controlled, double-blind or open-label trials, demonstrated that alteplase, when given at a dose of up to 2 mg/2 mL for up to two administrations, each followed by a dwell time of up to 120 minutes, is a safe and effective treatment for the restoration of catheter function in both adult and pediatric patients with occluded CVA catheters. Following administration of the first dose of alteplase, the rate of restoration of function to dysfunctional catheters after a dwell time of up to 120 minutes was 73.9%-76.5% for subjects 2 years of age and 69.1% for subjects <2 years of age. The rate of restoration of function following administration of up to two doses of alteplase was 83.5%-89.9% for subjects ≧2 years of age and 80.0% for subjects <2 years of age. A total of 39 of 1454 subjects (2.7%) reported serious adverse events during the three studies. All serious adverse events except three were judged to be unrelated to the alteplase. No ICHs, embolic events, or alteplase-related major bleeding were reported during the trials. The most common serious adverse event in these trials was sepsis/bacteremia (18%).

According to the United States Renal Data System, there were over 440,000 persons in the United States with end-stage renal disease at the end of 2003 (National Institutes of Health, U.S. Renal Data System. USRDS 2005 annual data report: atlas of end-stage renal disease in the United States. Bethesda (Md.): National Institutes of Health, National Institute of Diabetes and Digestive and Kidney Diseases (2005)). Of these, the vast majority underwent regular hemodialysis (HD), generally three times per week. Many of these patients receive HD through tunneled central venous catheters. For these patients, low catheter flow rates due to thrombotic obstruction of the lumens remain a frequent complication and have been estimated to affect 3%-10% of all HD sessions and 87% of all catheters at some time prior to their removal (Moss et al., Am J Kidney Dis; 12:492-8 (1988); Gibson and Mosquera, Nephrol Dial Transplant 1991;6:269-74 (1991); Suhocki et al., Am J Kidney Dis, 28:379-86 (1996)).

There is a need for using a fibrin-specific plasminogen activator efficaciously and uniformly to clear out HD catheters containing pathological collections of fluid. For example, there is a need for HD catheter-directed thrombolysis in a clinical setting that allows higher doses of tenecteplase than set forth in U.S. patent application Ser. No. 10/697,142 filed 30 Oct. 2003. Specifically, there is a need to administer a fibrin-specific plasminogen activator locally into the HD catheter lumen without systemic exposure to provide a way to salvage catheters with suboptimal flow rates while minimizing the risk of adverse events associated with systemic use of such agent. Because of the time constraints of HD sessions, there is a need for an agent such as tenecteplase, with high potency, high fibrin specificity, and efficiency to rapidly lyse clots. Furthermore, a continuing need exists for the prevention and removal of fibrin from such HD devices, as certain bacteria have binding sites that favor sticking to fibrin, in particular.

SUMMARY

Accordingly, the invention is as claimed. In one embodiment of the invention herein, a method is provided for restoring function in a dysfunctional hemodialysis catheter indwelling in a mammal, which catheter has a blood flow rate (BFR) of less than 300 mL/minute, which method comprises administering tenecteplase in a total dose of about 3 to 4 mg locally into all catheter lumens and allowing the tenecteplase to dwell in the catheter for from about one hour to about 72 hours, such that the flow rate of the catheter is no longer obstructed.

In one embodiment, the dysfunctional hemodialysis catheter additionally has a BFR at least 25 mg/ml below the prescribed BFR at an arterial pressure of -250 mmHg during the first 30 minutes of the hemodialysis.

Preferably, the tenecteplase is in a solution of sterile water for injection or bacteriostatic water for injection. Preferably, the tenecteplase dwells in the catheter until the BFR of the catheter is improved over the BFR before administration of tenecteplase and the improvement maintained for at least 48 hours. In other preferred embodiments, the tenecteplase is in sterile water for injection, and/or the tenecteplase is administered in a total dose of about 4 mg into all catheter lumens, wherein preferably about 2 mg/2 mL of tenecteplase is administered to each of two catheter lumens.

In other preferred aspects, the tenecteplase is instilled into the catheter for about one hour or as an extended dwell of from over about one hour to about 72 hours. Preferably, the dwell is from about 2 to about 48 hours. In another preferred aspect, the catheter is contacted with the solution for at least about five days to remove fibrin-bound blood clots.

In further preferred aspects, treatment may be repeated, i.e., the tenecteplase is administered more than once. One aspect of this procedure is that the tenecteplase is administered at each hemodialysis session that the mammal undergoes. In another preferred embodiment, no re-treatment is performed, i.e., the tenecteplase is administered only once or twice as an initial dose and then as an extended-dwell dose. Most preferably, the tenecteplase is administered only once, i.e., as one dose.

In other preferred aspects, the mammal undergoes hemodialysis after administration of the tenecteplase. In further embodiments, the mammal is a human.

In another aspect, a kit is provided comprising a container comprising a solution comprising tenecteplase, and instructions for using the solution to restore function in a dysfunctional hemodialysis catheter indwelling in a mammal, which catheter has a BFR of less than 300 mL/minute, which instructions direct the user to administer tenecteplase in a total dose of about 3 to 4 mg locally into all catheter lumens and allow the tenecteplase to dwell in the catheter for from about one hour to about 72 hours, such that the flow rate of the catheter is no longer obstructed.

In a further aspect, the invention concerns a method comprising manufacturing tenecteplase for restoring function in a dysfunctional hemodialysis catheter indwelling in a mammal, which catheter has a blood flow rate (BFR) of less than 300 mL/minute.

In a still further aspect, the invention concerns tenecteplase for use to restore function in a dysfunctional hemodialysis catheter indwelling in a mammal, which catheter has a blood flow rate (BFR) of less than 300 mL/minute.

The invention herein hence provides for using tenecteplase to treat hemodialysis catheters that are obstructed and become dysfunctional, particularly those that become dysfunctional due to pathological collections of fibrin-rich fluids residing in the catheter.

DESCRIPTION OF THE PREFERRED EMBODIMENTS
Definitions

As used herein, “hemodialysis catheter” or “HD catheter” refers to a dialysis catheter generally, but not necessarily, constructed of plastic polymers, e.g., polyurethane, silicone, or other polymers, that is useful in catheter-directed therapy (i.e., delivering medical therapy) to effect hemodialysis. The catheters herein are indwelling catheters, such as intravenous or arterial hemodialysis catheters, including those that are tunneled. The catheter preferably is not an implantable port, non-cuffed catheter, or non-tunneled catheter. The HD catheter is preferably not implanted in the jugular vein. Preferably, the HD catheter lumens doe not require flow reversal. Most preferred is a cuffed tunneled HD catheter. As used herein, a “dysfunctional” HD catheter is one that fails to attain and maintain an extracorporeal blood flow (≧300 mL/min) sufficient to perform HD without significantly lengthening HD treatment, as defined by the National Kidney Foundation, K/DOQI clinical practice guidelines for vascular access: updated 2000. Am J Kidney Dis 37:S137-81 (2001). Generally, such dysfunctional catheter has a BFR of less than 300 mL/minute typically at a maximum negative arterial pressure of 250 mmHg. Such dysfunctional catheters preferably show a demonstrated BFR of equal to or greater than 300 mL/minute in at least one HD session in the seven days prior to treatment by the method herein. HD catheters are not dysfunctional if they have a sustainable BFR of equal to or greater than 300 mL/minute following subject repositioning. The dysfunctional catheters herein preferably have no evidence of mechanical, non-thrombotic occlusion (e.g., a kink in the catheter or suture constricting the catheter), or occlusion caused by known fibrin sheath.

“Restoring function” means allowing HD to be carried out successfully at least once after treatment with the tenecteplase, that is, generally without obstruction and at the minimal flow rate to allow HD to proceed as prescribed by the physician. In generally, this means that function is restored when the catheter with suboptimal flow rates is salvaged and the BFR is restored to at least 300 mL/minute. While the subject must exhibit clinical treatment success at their first HD visit after treatment for restoration to occur, preferably the subject shows maintained catheter patency over a period of time beyond the first visit.

An indication of functional restoration beyond HD success is the percent improvement from baseline BFR at the end of HD administered at the first visit. The baseline

BFR is the BFR measurement obtained to determine if the patient is eligible for treatment. In one preferred embodiment, after a dwell time of the tenecteplase in the patient's catheter of about one hour, the tenecteplase instillation is discontinued and all patients undergo full HD. BFR is then generally measured during the last 30 minutes of HD to assess catheter function. In this preferred mode, subjects with a BFR of ≧300 mL/min continuously sustained for at least the last about 30 minutes and an increase from baseline BFR of ≧25 mL/min at the end of HD are considered a treatment success, and subjects with a BFR of ≧300 mL/min and an increase from baseline BFR of <25 mL/min and subjects with a BFR of <300 mL/min are considered to have had treatment failure. Also, in a preferred embodiment such subjects have a urea reduction ratio (URR) of at least about 65% as assessed by pre- and post-HD BUN measurements at the first HD visit after treatment with tenecteplase.

In another embodiment of functional restoration, after a dwell time of the tenecteplase in the patient's catheter of about one hour, the patient undergoes full HD, and BFR is measured during the last 30 minutes of HD to assess catheter function. Subjects with a BFR of ≧200 mL/min but <300 mL/min at the end of HD at the first visit get a second dose instilled for an extended dwell time, until the start of the second visit (up to 72 hours). The extended-dwell dose of tenecteplase is withdrawn from the catheter at the beginning of the second visit, and BFR is measured at the beginning of HD. Patients undergo full HD, and BFR is again measured during the last 30 minutes of HD. In this second preferred mode, subjects with a BFR of ≧300 mL/min continuously sustained for at least the last about 30 minutes and an increase from baseline BFR of ≧25 mL/min at the end of HD at the first or second visit are considered to be a treatment success. Those who have re-occlusion of their HD catheter (BFR of <300 mL/min) within 21 days of the first visit exit the initial treatment course and enter the retreatment course, during which they receive another dose of tenecteplase. After a dwell time of 1 hour, patients undergo full HD, and BFR is measured during the last 30 minutes of HD. In that case, patients with a BFR of 300 mL/min and an increase from baseline BFR of <25 mL/min and subjects with a BFR of <300 mL/min are considered to have had treatment and re-treatment failure.

“Administering” means infusing or instilling the drug into the catheter. This generally means that the lumen of the catheter is flushed with the tenecteplase. Allowing the tenecteplase to “dwell” means that the tenecteplase stays in the catheter to perform its function of restoring flow rate; such “dwell” generally means an intra-luminal dwell.

As used herein, a “pathological collection of a fibrin-rich fluid” refers to gathered fluids containing an excess of fibrin that cause problems in a hemodialysis catheter. The fluids may be from any source, including blood, cerebrospinal fluid, urine, and fluid from the peritoneal, pleural, or pericardial cavity, and, due to their high fibrin content, can be treated with a thrombolytic drug. Hence, this collection includes intra-vascular as well as non-vascular collections of fluid. This collection of fluid is contained in a hemodialysis catheter. This fluid is pathological preferably because it causes the hemodialysis catheter to be dysfunctional, thereby limiting effective hemodialysis. Effective hemodialysis is hemodialysis that will function properly for the subject being treated.

The term “mammal” for the purposes of treatment refers to any animal classified as a mammal, including but not limited to, humans, sport, zoo, pet, and domestic or farm animals, such as dogs, cats, cattle, sheep, pigs, horses, and primates, such as monkeys or humans. Preferably the mammal is a human. The mammal herein must require HD, and preferably must have been prescribed at a BFR of equal to or greater than 300 mL/minute. The mammals preferably have had their HD catheter inserted at least two days prior to their treatment. The eligible mammals also preferably use the same catheter for at least four consecutive HD sessions on the same type and model of HD apparatus. The mammal being treated preferably is able to have fluids infused at the volume necessary to instill the tenecteplase into the HD catheter. The mammal may be an adult or a pediatric mammal (e.g., for a human less than 18 years of age), but is preferably an adult, i.e., for a human at least 18 years old.

A “therapeutic composition” or “composition,” as used herein, is defined as comprising tenecteplase, sterile water for injection or bacteriostatic water for injection, as well as any optional pharmaceutically acceptable carrier(s), such as minerals, proteins, and other excipients known to one skilled in the art. Preferably, the tenecteplase is in the form of a lyophilized powder reconstituted in one of these types of waters.

As used herein, “solution” refers to a soluble mixture of ingredients, including complete solvation of the ingredients.

As used herein, the term “tenecteplase,” also known as TNK-tPA or TNKASE™ brand of tissue-plasminogen activator variant, refers to a tPA variant designated T103N, N117Q, K296A, H297A, R298A, R299A available from Genentech, Inc. wherein Thr103 of wild-type tPA is changed to Asn (T103N), Asn117 of wild-type tPA is changed to Gln (N117Q), and Lys-His-Arg-Arg (SEQ ID NO:1) 296-299 of wild-type tPA is changed to Ala-Ala-Ala-Ala (SEQ ID NO:2) (KHRR296-299AAAA). See the background section herein and U.S. Pat. No. 5,612,029.

As used herein, “sterile water for injection” or “SWFI” refers to the same substance as defined by the United States Pharmacopeia (USP), which is a sterile, non-pyrogenic preparation of water for injection that contains no bacteriostat, antimicrobial agent, or added buffer and is supplied only in single-dose containers to dilute or dissolve drugs for injection.

“Normal saline” refers to an aqueous solution of water containing 0.9% sodium chloride. It is also known as 0.9% sodium chloride injection USP, non-heparinized normal saline. Such saline is generally used clinically as a diluent for drugs administered by injection and as a plasma substitute.

“Bacteriostatic water for injection” or “BWFI” refers to a mixture of water and varying amounts of benzyl alcohol with no other ingredients as defined by the United States Pharmacopeia (USP).

Modes for Carrying Out the Invention

In one aspect of the invention herein, a method is provided for restoring function in a dysfunctional hemodialysis catheter indwelling in a mammal, which catheter has a BFR of less than 300 mL/minute, which method comprises administering tenecteplase in a total dose of about 3 to 4 mg locally into all catheter lumens (there are typically two lumens in the catheter) and allowing the tenecteplase to dwell in the catheter for from about one hour to about 72 hours, such that the flow rate of the catheter is no longer obstructed.

Preferably, the tenecteplase dwells in the catheter until the BFR of the catheter is improved over the BFR before administration of tenecteplase and the improvement maintained for at least 48 hours. In other preferred aspects, the tenecteplase is instilled into the catheter for about one hour or as an extended dwell of from over about one hour to about 72 hours. Preferably, the dwell is from about 2 to about 48 hours. In another preferred aspect, the catheter is contacted with the solution for at least about five days to remove fibrin-bound blood clots. In further embodiments, the tenecteplase may be administered once or more than once, and preferably only after HD sessions. Preferably, the mammal is a human.

Generally, screening and the first administration of tenecteplase is at the first visit by the subject for tenecteplase treatment followed by HD. The subjects are generally screened for eligibility based on the inclusion and exclusion criteria. Eligible subjects, with a BFR of <300 mL/min (all BFR measurements are preferably based on a maximum negative arterial pressure of 250 mmHg) at the beginning of HD (typically within the first 30 minutes), receive tenecteplase. The BFR measurement obtained to determine study eligibility is the baseline BFR.

In one embodiment, human patients preferably receive a concentration of tenecteplase of about 1 mg/mL, wherein the dose is about 2 mg/2 mL per lumen with a total dose of about 4 mg. In other words, the patient preferably receives a dose of about 2 mg/2 mL of tenecteplase, typically instilled into each of the two lumens of the HD catheter. Preferably after a dwell time of about one hour, the tenecteplase instillation is discontinued and all subjects undergo full HD. BFR is then generally measured during the last 30 minutes of HD to assess catheter function. In this preferred mode, subjects with a BFR of ≧300 mL/min continuously sustained for at least the last 30 minutes and an increase from baseline BFR of ≧25 mL/min at the end of HD are considered a treatment success, and subjects with a BFR of ≧300 mL/min and an increase from baseline BFR of <25 mL/min and subjects with a BFR of <300 mL/min are considered to have had treatment failure.

In this situation, subjects with a BFR of ≧300 mL/min at the end of HD at the first visit are preferably not further treated. Subjects with a BFR of <300 mL/min at the end of HD at the first visit are preferably treated with 2 mL (2 mg) of tenecteplase at the beginning of the next HD session if their BFR is still <300 mL/min at that time. After a dwell time of one hour, preferably the tenecteplase is discontinued and subjects undergo full HD. BFR is again measured during the last 30 minutes of HD to assess catheter function.

In this one preferred embodiment, subjects with treatment success at the first or second HD visit are assessed for HD catheter patency by measuring BFR at the beginning of HD (within the first 30 minutes) at each of the two visits that follow final tenecteplase exposure (i.e., the second and third visits for subjects who receive one dose of tenecteplase and the third and fourth visits for subjects who receive two doses of tenecteplase).

In a second preferred embodiment, the human patients receive up to three doses of tenecteplase. Subjects will receive one or two doses during an initial treatment course, and eligible subjects who experience re-occlusion of their catheter within 21 days of the first visit will receive an additional dose as part of a retreatment course.

Specifically, the patients are screened and treated at the first visit of the initial treatment course. The patients are screened for eligibility based on the inclusion and exclusion criteria. Eligible subjects, with a BFR of <300 mL/min (all BFR measurements are based on a maximum negative arterial pressure of 250 mmHg) at the beginning of HD (within the first 30 minutes), are treated with tenecteplase. The baseline BFR is as defined above. The patients are dosed with 2 mL (2 mg) of tenecteplase instilled into each of the two lumens of the HD catheter. After a dwell time of one hour, the tenecteplase is withdrawn and all patients undergo full HD. BFR is measured during the last 30 minutes of HD to assess catheter function. Patients with a BFR of ≧300 mL/min continuously sustained for at least the last 30 minutes and an increase from baseline BFR of ≧25 mL/min at the end of HD are considered to have had treatment success. Subjects with a BFR of ≧300 mL/min and an increase from baseline BFR of <25 mL/min and subjects with a BFR of <300 mL/min are considered to have had treatment failure.

Subjects with a BFR of <200 mL/min at the end of HD at the first visit, or a BFR of ≧300 mL/min and an increase from baseline BFR of <25 mL/min, are no longer treated. Subjects with a BFR of ≧200 mL/min but <300 mL/min at the end of HD at the first visit have 2 mL (2 mg) of tenecteplase instilled into each lumen of their catheter as part of the initial treatment course. The dose is left to dwell for an extended time, until the second HD session at the second visit (up to about 72 hours later). Patients who receive the extended-dwell dose of tenecteplase have the dose withdrawn from their catheter at the beginning of the second visit and then have BFR measured at the beginning of HD (within the first 30 minutes). Subjects undergo full HD, and BFR is again measured during the last 30 minutes of HD.

Subjects who have treatment success at the first or second visit and have re-occlusion of their HD catheter (BFR of <300 mL/min) within 21 days of the first visit discontinue the initial treatment and enter a retreatment course during which they again have 2 mL (2 mg) of tenecteplase instilled into each lumen, followed by a one-hour dwell time (at retreatment Visit 1).

Subjects who have treatment success at the first or second visit, or Retreatment Visit 1 are assessed for HD catheter patency by measuring BFR at the beginning of HD (within the first 30 minutes) at each of the two visits that follow final tenecteplase exposure.

This second option is designed to assess the efficacy of serial administration of up to three doses of tenecteplase for restoration of function to dysfunctional HD catheters, whereas the first option assesses efficacy of serial administration of up to two doses.

Hence, the invention herein includes not only administering a first dose of tenecteplase to those subjects requiring restoring of function of their hemodialysis catheters, but also administering subsequent doses of tenecteplase, typically in the same amount, but the amounts can differ. This treatment with multiple doses or re-treatment can be done once or several times, for example, at the beginning of each HD session. It may be done as many times as needed to ensure catheter patency and successful HD. Preferably, the tenecteplase is dosed only once or twice (as an initial instill and/or as an extended-dwell dose), and most preferred only once.

The tenecteplase may be administered in the form of a stable solution comprising tenecteplase and an appropriate form of water, especially sterile water for injection or bacteriostatic water for injection, along with any optional ingredients such as normal saline. While the tenecteplase solution useful herein may be prepared in any way, it is preferably prepared by reconstituting a lyophilized powder of tenecteplase in sterile water for injection or bacteriostatic water for injection. The tenecteplase is preferably administered in a total dose of about 4 mg into all catheter lumens, preferably two lumens. Most preferably, the tenecteplase is in sterile water for injection.

The amount of tenecteplase provided is that which will effect lyse any clots that occlude the catheter and otherwise restore function in dysfunctional hemodialysis catheters in a clinical or medical setting (with clinical and technical endpoints such as those set forth above in the definition section), but will not exceed that which would be a dangerous level in vivo so as to cause complications. Examples of major adverse events include intracranial hemorrhages (ICHs), major bleeding, embolic events, thrombosis, catheter-related bloodstream infections (CRBSIs), and catheter-related complications, as well as any procedure-related adverse event requiring additional procedures. Examples of minor bleeding complications include an access site hematoma greater than 5 cm that did not require any specific treatments or bleeding at any site and/or that was managed conservatively without the need for transfusion, evacuation, or prolongation of hospital stay.

According to the invention herein, reconstituted tenecteplase is formulated in a concentration of about 0.75 to 1 mg/mL to provide a dose of about 1.5 mg/2 mL to 2 mg/ 2 mL per catheter lumen, preferably in one of the waters as noted herein and optionally with other ingredients. Most preferably, the tenecteplase is formulated at a concentration of about 1 mg/mL (to provide a dose of about 2 mL of 2 mg of tenecteplase per lumen).

Compositions particularly well suited for the clinical administration of the tenecteplase used to practice this invention include sterile aqueous solutions or sterile hydratable powders such as lyophilized protein. Preferably, this formulation is derived from a lyophilized powder of tenecteplase that is reconstituted in water, preferably sterile water for injection or bacteriostatic water for injection. A buffer such as arginine base in combination with phosphoric acid is also typically included at an appropriate concentration to maintain a suitable pH, generally from 5.5 to 7.5. In addition or alternatively, a compound such as glycerol may be included in the formulation to help maintain the shelf-life. The formulation preferably comprises arginine, phosphoric acid, and an emulsifying agent such as a polyoxyethylene sorbitan fatty ester such as POLYSORBATE 20™ polyoxyethylene 20 sorbitan monolaurate, POLYSORBATE 80™ polyethylene sorbitan monooleate, or POLYSORBATE 65™ polyoxyethylene 20 sorbitan tristearate, which, in some embodiments, accompany the tenecteplase that is lyophilized.

In a less preferred embodiment, an appropriate amount of a pharmaceutically acceptable salt is also used in the formulation to render the formulation isotonic. For example, a non-lyophilized sterile solution might optionally, but not preferably, contain normal saline.

Tenecteplase is commercially available as a sterile, preservative-free, lyophilized powder in a vial containing 52.5 mg of tenecteplase, 0.55 g of L-arginine, 0.17 g of phosphoric acid, 4.3 mg of POLYSORBATE 20™ polyoxyethylene 20 sorbitan monolaurate supplied with a 10-mL syringe of sterile water for injection USP. Alternatively, the tenecteplase can be supplied with a 10-mL syringe of bacteriostatic water for injection. The preferred water for injection herein is sterile water for injection.

As one example of an appropriate dosage form, a vial containing about 50 mg of tenecteplase, as well as arginine, phosphoric acid, and a POLYSORBATE™ emulsifier is reconstituted with 50 mL of sterile water for injection.

In another embodiment, to reconstitute the product, about 10 mL of preservative-free sterile water for injection USP is mixed with the tenecteplase powder under sterile conditions to produce a final concentration of about 1 mg/mL. Alternatively, tenecteplase is reconstituted to a concentration of about 1 mg/mL in BWFI (0.9%) with full viability of protein. Unused reconstituted tenecteplase may be stored at controlled room temperature (15-30° C.) for up to 8 hours or under refrigeration (2-8° C.) for 24 hours.

In a small-vial configuration, a vial may contain 2 mg of tenecteplase in 2 mL of the water for injection. Vials with weights and volumes in between about 1 mg and 4 mg and between about 1 mL and 4 mL, respectively, are also contemplated herein.

Since the procedures herein using tenecteplase involve total doses of about 2-3 mg for catheter clearance, the reconstituted tenecteplase may be readily frozen for later use. Many institutions are reconstituting and freezing smaller aliquots (2- and 5-mL syringes) of tenecteplase for future use to minimize waste and decrease costs.

Visual inspection of the solution for precipitates is recommended after dilution and before administration. Tenecteplase is preservative-free and is theoretically susceptible to bacterial contamination and biochemical degradation when left at room temperature for more than 8 hours. Although the manufacturer recommends changing the solution after 24 hours, the drug should be physically and chemically stable for 24 hours.

The tenecteplase may be instilled into the catheter for up to about one hour or for about one hour, or may be instilled longer as an extended dwell of from over about one hour to about 72 hours, preferably about 2 hours to 48 hours. More than about 72 hours may also be needed. Preferably, the amount is about one hour or up to about 24 hours. If fibrin-bound blood clots are being removed from a catheter, the catheter may be contacted with the solution herein for at least about 5 days, preferably about 6 to 15 days.

The tenecteplase solution herein may be instilled or infused into the catheter by any suitable technique. The skilled practitioner would be easily able to devise methods of administration of the solution herein based on the general knowledge in the literature on lytic administration.

The effects of administration of tenecteplase can be measured by a variety of assays known in the art, as noted in the definitions above, such as the percent improvement from baseline BFR at the end of HD at the first visit, the urea reduction ratio as assessed by pre- and post-HD BUN measurements, the success of HD treatment following the lytic indwelling, etc. Physicians should continue to use the catheter-based modality with which they are most comfortable.

Risk factors for adverse bleeding with tenecteplase are similar to those associated with alteplase, UK, and other plasminogen activators. Variables associated with adverse bleeding risks include increased tenecteplase dose, duration of infusion, adjunctive anti-thrombotic therapy (e.g., heparin, aspirin, or other anti-platelet agents as noted herein), hypertension, increasing age, severity of ischemia, and female gender. Physicians should be aware of these risk factors and use appropriate caution during treatment. If adverse bleeding occurs during infusion therapy, tenecteplase should be immediately terminated and blood products (fresh frozen plasma or cryoprecipitate) administered to reverse hypocoagulability.

The tenecteplase is preferably administered without any other active drug. However, the invention includes circumstances wherein an active drug other than tenecteplase is infused into the catheter. Examples of such co-agents include blood thinners such as heparin and heparin analogs including low-molecular-weight heparin such as tinzaparin, certoparin, parnaparin, nadroparin, ardeparin, enoxaparin (LOVENOX™, Aventis Pharma, Bridgewater, N.J.), reviparin, reviparin and dalteparin, warfarin (3-(alpha-acetonylbenzyl)-4-hydroxycoumarin, or COUMADIN®), or aspirin; anti-coagulants such as tPA; tPA variants such as reteplase; urokinase; streptokinase; and alfimeprase.

Other drugs may be administered directly to the subject while undergoing HD treatment and administration of tenecteplase. However, it is preferable if no other thrombolytics are administered directly to the patient during this time.

These co-agents may be administered to the catheter by a route and in an amount commonly used therefor, contemporaneously or sequentially with the tenecteplase. When the tenecteplase is used contemporaneously with one or more other drugs, a pharmaceutical unit dosage form containing such other drugs in addition to the tenecteplase is preferred. Tenecteplase is incompatible and may precipitate when mixed directly with unfractionated heparin; concomitant heparin should be given by a separate means. An opaque diluent indicates precipitation of drug and may be associated with decreased efficacy. Such additional molecules are suitably present or administered in combination in amounts that are effective for the purpose intended, typically less than what is used if they are administered alone without the tenecteplase.

The invention also provides kits. In one embodiment, the kit comprises a container comprising a solution that contains at least tenecteplase (preferably in sterile water for injection or bacteriostatic water for injection), and instructions for using the solution to restore function in a dysfunctional hemodialysis catheter indwelling in a mammal, which catheter has a BFR of less than 300 mL/minute, which instructions direct the user to administer tenecteplase in a total dose of about 3 to 4 mg locally into all catheter lumens and allow the tenecteplase to dwell in the catheter for from about one hour to about 72 hours, such that the flow rate of the catheter is no longer obstructed. The preferred embodiments of the instruction guidelines are noted above for the method of restoration.

The kit may also comprise instructions for re-administration. It may also comprise a further container with a co-agent, as defined above, as active ingredient with instructions for co-administration thereof in an effective amount with the solution. A preferred such embodiment is a container comprising abciximab, eptifibatide, tirofiban hydrochloride, heparin, or warfarin with instructions for co-administration thereof in an effective amount with the diluted solution.

These further instructions included with the kit generally include information as to dosage, dosing schedule, and other guidance for the treatment of the HD catheter. The containers of tenecteplase may be unit doses, bulk packages (e.g., multi-dose packages), or sub-unit doses.

In the kit, tenecteplase may be packaged in any convenient, appropriate packaging. For example, if the tenecteplase is a freeze-dried formulation, an ampoule or vial with a resilient stopper is preferably used as the container, so that the drug may be easily reconstituted by injecting fluid through the resilient stopper. Ampoules with non-resilient, removable closures (e.g., sealed glass) or resilient stoppers are most conveniently used for solutions of tenecteplase ready for use in the catheter. In this latter case, the instructions preferably specify placing the contents of the vial in a catheter for immediate delivery.

Various features and aspects of the present invention are illustrated further in the examples that follow. While these examples are presented to show one skilled in the art how to operate within the scope of the invention, they are not intended in any way to serve as a limitation upon the scope of the invention. The disclosure of all citations herein is expressly incorporated herein by reference.

EXAMPLE 1

The goal of the study set forth in this Example is to examine the efficacy and safety of tenecteplase in the restoration of function to dysfunctional HD catheters, compared with a placebo control.

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